多囊肾病的产前诊断：诊断率、新的致病变异体以及基因型-表型相关性。

Prenatal diagnosis of polycystic renal diseases: diagnostic yield, novel disease-causing variants, and genotype-phenotype correlations.

机构信息

Prenatal Diagnostic Center, Guangzhou Women and Children's Medical Center, Guangzhou Medical University, Guangzhou, China (Mr Huang, Dr Fu, Mr Guo, Mr Zhou, Ms Yu, Dr Yan, Ms Liu, Dr Lu, Ms Ma, Ms Y Wang, Ms Chen, Dr D Wang, Ms Zhang, Ms Jing, Dr F Li, Dr Han, Dr D Li, Dr R Li, and Ms Liao).

出版信息

Am J Obstet Gynecol MFM. 2024 Jan;6(1):101228. doi: 10.1016/j.ajogmf.2023.101228. Epub 2023 Nov 18.

DOI:10.1016/j.ajogmf.2023.101228

PMID:37984685

Abstract

BACKGROUND

Polycystic renal disease is a frequent congenital anomaly of the kidneys, but research using chromosomal microarray analysis and exome sequencing in fetuses with polycystic renal disease remains sparse, with most studies focusing on the multisystem or genitourinary system.

OBJECTIVE

This study aimed to assess the detection rate of detectable genetic causes of fetal polycystic renal disease at different levels, novel disease-causing variants, and genotype-phenotype correlations.

STUDY DESIGN

This study included 220 fetal polycystic renal disease cases from January 2014 to June 2022. Cases were divided into the following 3 groups: isolated multicystic dysplastic kidneys, nonisolated multicystic dysplastic kidneys, and suspected polycystic kidney disease group. We reviewed data on maternal demographics, ultrasonographic results, chromosomal microarray analysis/exome sequencing results, and pregnancy outcomes.

RESULTS

In our cohort, chromosomal microarray analysis identified 19 (8.6%) fetuses carrying chromosomal abnormalities, and the most common copy number variation was 17q12 microdeletion (7/220; 3.2%). Furthermore, 94 families chose to perform trio-exome sequencing testing, and 21 fetuses (22.3%) were found to harbor pathogenic/likely pathogenic variants. There was a significant difference in the live birth rate among the 3 groups (91/130 vs 46/80 vs 1/10; P<.001). Among 138 live birth cases, 106 (78.5%) underwent postnatal ultrasound review, of which 95 (89.6%) had a consistent prenatal-postnatal ultrasound diagnosis.

CONCLUSION

For both isolated and nonisolated polycystic renal disease, our data showed high detection efficiency with both testing tools. The detection of novel pathogenic variants expands the known disease spectrum of polycystic renal disease-associated genes while enriching our understanding of the genotype-phenotype correlation. Therefore, we consider it feasible to perform chromosomal microarray analysis+exome sequencing testing in fetal polycystic renal disease. Moreover, prenatal-postnatal ultrasound concordance was greater, the live birth rate was higher, and prognosis was better when known genetic disorders were excluded, indicating that genetic testing results significantly influenced pregnancy decisions.

摘要

背景

多囊肾病是一种常见的肾脏先天性异常，但使用染色体微阵列分析和外显子组测序研究多囊肾病胎儿的研究仍然很少，大多数研究集中在多系统或泌尿生殖系统。

目的

本研究旨在评估不同水平检测胎儿多囊肾病可检测遗传原因的检出率、新的致病变异体以及基因型-表型相关性。

研究设计

本研究纳入了 2014 年 1 月至 2022 年 6 月期间 220 例多囊肾病胎儿。病例分为以下 3 组：孤立性多囊性发育不良肾、非孤立性多囊性发育不良肾和疑似多囊肾病组。我们回顾了母体人口统计学数据、超声结果、染色体微阵列分析/外显子组测序结果和妊娠结局。

结果

在我们的队列中，染色体微阵列分析发现 19 例（8.6%）胎儿携带染色体异常，最常见的拷贝数变异是 17q12 微缺失（7/220；3.2%）。此外，94 个家庭选择进行三体外显子组测序检测，发现 21 例（22.3%）胎儿携带致病性/可能致病性变异体。3 组间的活产率有显著差异（91/130 比 46/80 比 1/10；P<.001）。在 138 例活产病例中，106 例（78.5%）进行了产后超声复查，其中 95 例（89.6%）产前-产后超声诊断一致。

结论

对于孤立性和非孤立性多囊肾病，我们的数据显示两种检测工具都具有较高的检测效率。新致病变异体的发现扩展了多囊肾病相关基因的已知疾病谱，同时丰富了我们对基因型-表型相关性的理解。因此，我们认为在胎儿多囊肾病中进行染色体微阵列分析+外显子组测序检测是可行的。此外，排除已知遗传疾病时，产前-产后超声一致性更高、活产率更高、预后更好，表明遗传检测结果显著影响妊娠决策。